Brand Name:Tenormin
Generic Name: Atenolol
Tenormin (Atenolol) is a beta blocker medication used in treatment of blood
pressure, angina pectoris, heart attack and anxiety. Detailed info on uses, dosage and side-effects of
Tenormin below.
Contents:
Description
Pharmacology
Indications and Usage
Contraindications
Warnings
Precautions
Drug Interactions
Adverse Reactions
Overdose
Dosage
Supplied
DESCRIPTION TENORMIN® (atenolol), a synthetic, beta 1 -selective (cardioselective)
adrenoreceptor blocking agent, may be chemically described as benzeneacetamide,
4-[2'-hydroxy-3'-[(1-methylethyl) amino] propoxy]-. The molecular and structural
formulas are:
Atenolol (free base) has a molecular weight of 266. It is a relatively polar
hydrophilic compound with a water solubility of 26.5 mg/mL at 37°C and a log
partition coefficient (octanol/water) of 0.23. It is freely soluble in 1N HCl
(300 mg/mL at 25°C) and less soluble in chloroform (3 mg/mL at 25°C).
TENORMIN is available as 25, 50 and 100 mg tablets for oral administration.
Inactive Ingredients: Magnesium stearate, microcrystalline cellulose,
povidone, sodium starch glycolate.
TENORMIN is a beta 1 -selective (cardioselective) beta-adrenergic receptor
blocking agent without membrane stabilizing or intrinsic sympathomimetic
(partial agonist) activities. This preferential effect is not absolute, however,
and at higher doses, TENORMIN inhibits beta 2 -adrenoreceptors, chiefly located
in the bronchial and vascular musculature.
Pharmacokinetics and Metabolism:
In man, absorption of an oral dose is rapid and consistent but incomplete.
Approximately 50% of an oral dose is absorbed from the gastrointestinal tract,
the remainder being excreted unchanged in the feces. Peak blood levels are
reached between two (2) and four (4) hours after ingestion. Unlike propranolol
or metoprolol, but like nadolol, TENORMIN undergoes little or no metabolism by
the liver, and the absorbed portion is eliminated primarily by renal excretion.
Over 85% of an intravenous dose is excreted in urine within 24 hours compared
with approximately 50% for an oral dose. TENORMIN also differs from propranolol
in that only a small amount (6%-16%) is bound to proteins in the plasma. This
kinetic profile results in relatively consistent plasma drug levels with about a
fourfold interpatient variation.
The elimination half-life of oral TENORMIN is approximately 6 to 7 hours, and
there is no alteration of the kinetic profile of the drug by chronic
administration. Following intravenous administration, peak plasma levels are
reached within 5 minutes. Declines from peak levels are rapid (5- to 10-fold)
during the first 7 hours; thereafter, plasma levels decay with a half-life
similar to that of orally administered drug. Following oral doses of 50 mg or
100 mg, both beta-blocking and antihypertensive effects persist for at least 24
hours. When renal function is impaired, elimination of TENORMIN is closely
related to the glomerular filtration rate; significant accumulation occurs when
the creatinine clearance falls below 35 mL/min/1.73m 2 . (See DOSAGE AND
ADMINISTRATION.)
Pharmacodynamics:
In standard animal or human pharmacological tests, beta-adrenoreceptor
blocking activity of TENORMIN has been demonstrated by: (1) reduction in resting
and exercise heart rate and cardiac output, (2) reduction of systolic and
diastolic blood pressure at rest and on exercise, (3) inhibition of
isoproterenol induced tachycardia, and (4) reduction in reflex orthostatic
tachycardia.
A significant beta-blocking effect of TENORMIN, as measured by reduction of
exercise tachycardia, is apparent within one hour following oral administration
of a single dose. This effect is maximal at about 2 to 4 hours, and persists for
at least 24 hours. Maximum reduction in exercise tachycardia occurs within 5
minutes of an intravenous dose. For both orally and intravenously administered
drug, the duration of action is dose related and also bears a linear
relationship to the logarithm of plasma TENORMIN concentration. The effect on
exercise tachycardia of a single 10 mg intravenous dose is largely dissipated by
12 hours, whereas beta-blocking activity of single oral doses of 50 mg and 100
mg is still evident beyond 24 hours following administration. However, as has
been shown for all beta-blocking agents, the antihypertensive effect does not
appear to be related to plasma level.
In normal subjects, the beta 1 selectivity of TENORMIN has been shown by its
reduced ability to reverse the beta 2 -mediated vasodilating effect of
isoproterenol as compared to equivalent beta-blocking doses of propranolol. In
asthmatic patients, a dose of TENORMIN producing a greater effect on resting
heart rate than propranolol resulted in much less increase in airway resistance.
In a placebo controlled comparison of approximately equipotent oral doses of
several beta blockers, TENORMIN produced a significantly smaller decrease of FEV
1 than nonselective beta blockers such as propranolol and, unlike those agents,
did not inhibit bronchodilation in response to isoproterenol.
Consistent with its negative chronotropic effect due to beta blockade of the
SA node, TENORMIN increases sinus cycle length and sinus node recovery time.
Conduction in the AV node is also prolonged. TENORMIN is devoid of membrane
stabilizing activity, and increasing the dose well beyond that producing beta
blockade does not further depress myocardial contractility. Several studies have
demonstrated a moderate (approximately 10%) increase in stroke volume at rest
and during exercise.
In controlled clinical trials, TENORMIN, given as a single daily oral dose,
was an effective antihypertensive agent providing 24-hour reduction of blood
pressure. TENORMIN has been studied in combination with thiazide-type diuretics,
and the blood pressure effects of the combination are approximately additive.
TENORMIN is also compatible with methyldopa, hydralazine, and prazosin, each
combination resulting in a larger fall in blood pressure than with the single
agents. The dose range of TENORMIN is narrow and increasing the dose beyond 100
mg once daily is not associated with increased antihypertensive effect. The
mechanisms of the antihypertensive effects of beta-blocking agents have not been
established. Several possible mechanisms have been proposed and include: (1)
competitive antagonism of catecholamines at peripheral (especially cardiac)
adrenergic neuron sites, leading to decreased cardiac output, (2) a central
effect leading to reduced sympathetic outflow to the periphery, and (3)
suppression of renin activity. The results from long-term studies have not shown
any diminution of the antihypertensive efficacy of TENORMIN with prolonged use.
By blocking the positive chronotropic and inotropic effects of catecholamines
and by decreasing blood pressure, atenolol generally reduces the oxygen
requirements of the heart at any given level of effort, making it useful for
many patients in the long-term management of angina pectoris. On the other hand,
atenolol increase oxygen requirements by increasing left ventricular fiber
length and end diastolic pressure, particularly in patients with heart failure.
In a multicenter clinical trial (ISIS-1) conducted in 16,027 patients with
suspected myocardial infarction, patients presenting within 12 hours (mean = 5
hours) after the onset of pain were randomized to either conventional therapy
plus TENORMIN (n = 8,037), or conventional therapy alone (n = 7,990). Patients
with a heart rate of < 50 bpm or systolic blood pressure < 100 mm Hg, or with
other contraindications to beta blockade were excluded. Thirty-eight percent of
each group were treated within 4 hours of onset of pain. The mean time from
onset of pain to entry was 5.0 ± 2.7 hours in both groups. Patients in the
TENORMIN group were to receive TENORMIN I.V. Injection 5-10 mg given over 5
minutes plus TENORMIN Tablets 50 mg every 12 hours orally on the first study day
(the first oral dose administered about 15 minutes after the IV dose) followed
by either TENORMIN Tablets 100 mg once daily or TENORMIN Tablets 50 mg twice
daily on days 2-7. The groups were similar in demographic and medical history
characteristics and in electrocardiographic evidence of myocardial infarction,
bundle branch block, and first degree atrioventricular block at entry.
During the treatment period (days 0-7), the vascular mortality rates were
3.89% in the TENORMIN group (313 deaths) and 4.57% in the control group (365
deaths). This absolute difference in rates, 0.68%, is statistically significant
at the P < 0.05 level. The absolute difference translates into a proportional
reduction of 15% (3.89-4.57/4.57 = -0.15). The 95% confidence limits are 1%-27%.
Most of the difference was attributed to mortality in days 0-1 (TENORMIN - 121
deaths; control - 171 deaths).
Despite the large size of the ISIS-1 trial, it is not possible to identify
clearly subgroups of patients most likely or least likely to benefit from early
treatment with atenolol. Good clinical judgment suggests, however, that patients
who are dependent on sympathetic stimulation for maintenance of adequate cardiac
output and blood pressure are not good candidates for beta blockade. Indeed, the
trial protocol reflected that judgment by excluding patients with blood pressure
consistently below 100 mm Hg systolic. The overall results of the study are
compatible with the possibility that patients with borderline blood pressure
(less than 120 mm Hg systolic), especially if over 60 years of age, are less
likely to benefit.
The mechanism through which atenolol improves survival in patients with
definite or suspected acute myocardial infarction is unknown, as is the case for
other beta blockers in the postinfarction setting. Atenolol, in addition to its
effects on survival, has shown other clinical benefits including reduced
frequency of ventricular premature beats, reduced chest pain, and reduced enzyme
elevation.
Atenolol Geriatric Pharmacology:
In general, elderly patients present higher atenolol plasma levels with total
clearance values about 50% lower than younger subjects. The half-life is
markedly longer in the elderly compared to younger subjects. The reduction in
atenolol clearance follows the general trend that the elimination of renally
excreted drugs is decreased with increasing age.
Hypertension:
TENORMIN is indicated in the management of hypertension. It may be used alone
or concomitantly with other antihypertensive agents, particularly with a
thiazide-type diuretic.
Angina Pectoris Due to Coronary Atherosclerosis:
TENORMIN is indicated for the long-term management of patients with angina
pectoris.
Acute Myocardial Infarction:
TENORMIN is indicated in the management of hemodynamically stable patients
with definite or suspected acute myocardial infarction to reduce cardiovascular
mortality. Treatment can be initiated as soon as the patient's clinical
condition allows. (See DOSAGE AND ADMINISTRATION ,
CONTRAINDICATIONS , and
WARNINGS .) In general, there is no basis for treating patients like those
who were excluded from the ISIS-1 trial (blood pressure less than 100 mm Hg
systolic, heart rate less than 50 bpm) or have other reasons to avoid beta
blockade. As noted above, some subgroups (eg, elderly patients with systolic
blood pressure below 120 mm Hg) seemed less likely to benefit.
TENORMIN is contraindicated in sinus bradycardia, heart block greater than
first degree, cardiogenic shock, and overt cardiac failure. (See
WARNINGS.)
TENORMIN is contraindicated in those patients with a history of
hypersensitivity to the atenolol or any of the drug product's components.
Cardiac Failure: Sympathetic stimulation is necessary in supporting
circulatory function in congestive heart failure, and beta blockade carries the
potential hazard of further depressing myocardial contractility and
precipitating more severe failure. In patients who have congestive heart failure
controlled by digitalis and/or diuretics, TENORMIN should be administered
cautiously. Both digitalis and atenolol slow AV conduction.
In patients with acute myocardial infarction, cardiac failure which is not
promptly and effectively controlled by 80 mg of intravenous furosemide or
equivalent therapy is a contraindication to beta-blocker treatment.
In Patients Without a History of Cardiac Failure: Continued depression
of the myocardium with beta-blocking agents over a period of time can, in some
cases, lead to cardiac failure. At the first sign or symptom of impending
cardiac failure, patients should be treated appropriately according to currently
recommended guidelines, and the response observed closely. If cardiac failure
continues despite adequate treatment, TENORMIN should be withdrawn. (See
DOSAGE AND ADMINISTRATION)
Cessation of Therapy with TENORMIN:
Patients with coronary artery disease, who are being treated with
TENORMIN, should be advised against abrupt discontinuation of therapy.
Severe exacerbation of angina and the occurrence of myocardial
infarction and ventricular arrhythmias have been reported in angina
patients following the abrupt discontinuation of therapy with beta
blockers. The last two complications may occur with or without preceding
exacerbation of the angina pectoris. As with other beta blockers, when
discontinuation of TENORMIN is planned, the patients should be carefully
observed and advised to limit physical activity to a minimum. If the
angina worsens or acute coronary insufficiency develops, it is
recommended that TENORMIN be promptly reinstituted, at least
temporarily. Because coronary artery disease is common and may be
unrecognized, it may be prudent not to discontinue TENORMIN therapy
abruptly even in patients treated only for hypertension. (See
DOSAGE AND ADMINISTRATION.) |
Concomitant Use of Calcium Channel Blockers: Bradycardia and heart
block can occur and the left ventricular end diastolic pressure can rise when
beta-blockers are administered with verapamil or diltiazem. Patients with
preexisting conduction abnormalities or left ventricular dysfunction are
particularly susceptible. (See PRECAUTIONS.)
Bronchospastic Diseases:
PATIENTS WITH BRONCHOSPASTIC DISEASE SHOULD, IN GENERAL, NOT RECEIVE BETA
BLOCKERS. Because of its relative beta 1 selectivity, however, TENORMIN may be
used with caution in patients with bronchospastic disease who do not respond to,
or cannot tolerate, other antihypertensive treatment. Since beta 1 selectivity
is not absolute, the lowest possible dose of TENORMIN should be used with
therapy initiated at 50 mg and a beta 2 -stimulating agent (bronchodilator)
should be made available. If dosage must be increased, dividing the dose should
be considered in order to achieve lower peak blood levels.
Anesthesia and Major Surgery: It is not advisable to withdraw beta-adrenoreceptor
blocking drugs prior to surgery in the majority of patients. However, care
should be taken when using anesthetic agents such as those which may depress the
myocardium. Vagal dominance, if it occurs, may be corrected with atropine (1-2
mg IV).
TENORMIN, like other beta blockers, is a competitive inhibitor of
beta-receptor agonists and its effects on the heart can be reversed by
administration of such agents: eg, dobutamine or isoproterenol with caution (see
section on OVERDOSAGE).
Diabetes and Hypoglycemia: TENORMIN should be used with caution in
diabetic patients if a beta-blocking agent is required. Beta blockers may mask
tachycardia occurring with hypoglycemia, but other manifestations such as
dizziness and sweating may not be significantly affected. At recommended doses
TENORMIN does not potentiate insulin-induced hypoglycemia and, unlike
nonselective beta blockers, does not delay recovery of blood glucose to normal
levels.
Thyrotoxicosis: Beta-adrenergic blockade may mask certain clinical
signs (eg, tachycardia) of hyperthyroidism. Abrupt withdrawal of beta blockade
might precipitate a thyroid storm; therefore, patients suspected of developing
thyrotoxicosis from whom TENORMIN therapy is to be withdrawn should be monitored
closely. (See DOSAGE AND ADMINISTRATION.)
Untreated Pheochromocytoma: TENORMIN should not be given to patients
with untreated pheochromocytoma.
Pregnancy and Fetal Injury: Atenolol can cause fetal harm when
administered to a pregnant woman. Atenolol crosses the placental barrier and
appears in cord blood. Administration of atenolol, starting in the second
trimester of pregnancy, has been associated with the birth of infants that are
small for gestational age. No studies have been performed on the use of atenolol
in the first trimester and the possibility of fetal injury cannot be excluded.
If this drug is used during pregnancy, or if the patient becomes pregnant while
taking this drug, the patient should be apprised of the potential hazard to the
fetus.
Neonates born to mothers who are receiving TENORMIN at parturition or
breast-feeding may be at risk for hypoglycemia and bradycardia. Caution should
be exercised when TENORMIN is administered during pregnancy or to a woman who is
breast-feeding. (See PRECAUTIONS, Nursing Mothers.)
Atenolol has been shown to produce a dose-related increase in embryo/fetal
resorptions in rats at doses equal to or greater than 50 mg/kg/day or 25 or more
times the maximum recommended human antihypertensive dose. * Although similar
effects were not seen in rabbits, the compound was not evaluated in rabbits at
doses above 25 mg/kg/day or 12.5 times the maximum recommended human
antihypertensive dose. *
*Based on the maximum dose of 100 mg/day in a 50 kg patient.
General
Patients already on a beta blocker must be evaluated carefully before
TENORMIN is administered. Initial and subsequent TENORMIN dosages can be
adjusted downward depending on clinical observations including pulse and blood
pressure. TENORMIN may aggravate peripheral arterial circulatory disorders.
Impaired Renal Function
The drug should be used with caution in patients with impaired renal
function. (See DOSAGE AND ADMINISTRATION.)
Drug Interactions
Catecholamine-depleting drugs (eg, reserpine) may have an additive effect
when given with beta-blocking agents. Patients treated with TENORMIN plus a
catecholamine depletor should therefore be closely observed for evidence of
hypotension and/or marked bradycardia which may produce vertigo, syncope, or
postural hypotension.
Calcium channel blockers may also have an additive effect when given with
TENORMIN (See WARNINGS.)
Beta blockers may exacerbate the rebound hypertension which can follow the
withdrawal of clonidine. If the two drugs are coadministered, the beta blocker
should be withdrawn several days before the gradual withdrawal of clonidine. If
replacing clonidine by beta-blocker therapy, the introduction of beta blockers
should be delayed for several days after clonidine administration has stopped.
Concomitant use of prostaglandin synthase inhibiting drugs, eg, indomethacin,
may decrease the hypotensive effects of beta blockers.
Information on concurrent usage of atenolol and aspirin is limited. Data from
several studies, ie, TIMI-II, ISIS-2, currently do not suggest any clinical
interaction between aspirin and beta blockers in the acute myocardial infarction
setting.
While taking beta blockers, patients with a history of anaphylactic reaction
to a variety of allergens may have a more severe reaction on repeated challenge,
either accidental, diagnostic or therapeutic. Such patients may be unresponsive
to the usual doses of epinephrine used to treat the allergic reaction.
Carcinogenesis, Mutagenesis, Impairment of Fertility:
Two long-term (maximum dosing duration of 18 or 24 months) rat studies and
one long-term (maximum dosing duration of 18 months) mouse study, each employing
dose levels as high as 300 mg/kg/day or 150 times the maximum recommended human
antihypertensive dose, * did not indicate a carcinogenic potential of atenolol.
A third (24 month) rat study, employing doses of 500 and 1,500 mg/kg/day (250
and 750 times the maximum recommended human antihypertensive dose * ) resulted
in increased incidences of benign adrenal medullary tumors in males and females,
mammary fibroadenomas in females, and anterior pituitary adenomas and thyroid
parafollicular cell carcinomas in males. No evidence of a mutagenic potential of
atenolol was uncovered in the dominant lethal test (mouse), in vivo cytogenetics
test (Chinese hamster) or Ames test ( S typhimurium ).
Fertility of male or female rats (evaluated at dose levels as high as 200
mg/kg/day or 100 times the maximum recommended human dose * ) was unaffected by
atenolol administration.
*Based on the maximum dose of 100 mg/day in a 50 kg patient.
Animal Toxicology:
Chronic studies employing oral atenolol performed in animals have revealed
the occurrence of vacuolation of epithelial cells of Brunner's glands in the
duodenum of both male and female dogs at all tested dose levels of atenolol
(starting at 15 mg/kg/day or 7.5 times the maximum recommended human
antihypertensive dose * ) and increased incidence of atrial degeneration of
hearts of male rats at 300 but not 150 mg atenolol/kg/day (150 and 75 times the
maximum recommended human antihypertensive dose, * respectively).
Usage in Pregnancy:
Pregnancy
Category D: See WARNINGS -- Pregnancy and Fetal
Injury .
Nursing Mothers:
Atenolol is excreted in human breast milk at a ratio of 1.5 to 6.8 when
compared to the concentration in plasma. Caution should be exercised when
TENORMIN is administered to a nursing woman. Clinically significant bradycardia
has been reported in breast-fed infants. Premature infants, or infants with
impaired renal function, may be more likely to develop adverse effects.
Neonates born to mothers who are receiving TENORMIN at parturition or
breast-feeding may be at risk for hypoglycemia. Caution should be exercised when
TENORMIN is administered during pregnancy or to a woman who is breast-feeding
(See WARNINGS, Pregnancy and Fetal Injury ).
Pediatric Use:
Safety and effectiveness in pediatric patients have not been established.
Geriatric Use:
Hypertension and Angina Pectoris Due to Coronary Atherosclerosis:
Clinical studies of TENORMIN did not include sufficient number of patients aged
65 and over to determine whether they respond differently from younger subjects.
Other reported clinical experience has not identified differences in responses
between the elderly and younger patients. In general, dose selection for an
elderly patient should be cautious, usually starting at the low end of the
dosing range, reflecting the greater frequency of decreased hepatic, renal, or
cardiac function, and of concomitant disease or other drug therapy.
Acute Myocardial Infarction:
Of the 8,037 patients with suspected acute myocardial infarction randomized to
TENORMIN in the ISIS-1 trial (See CLINICAL PHARMACOLOGY),
33% (2,644) were 65 years of age and older. It was not possible to identify
significant differences in efficacy and safety between older and younger
patients; however, elderly patients with systolic blood pressure < 120 mmHg
seemed less likely to benefit (See INDICATIONS AND USAGE).
In general, dose selection for an elderly patient should be cautious, usually
starting at the low end of the dosing range, reflecting greater frequency of
decreased hepatic, renal, or cardiac function, and of concomitant disease or
other drug therapy. Evaluation of patients with hypertension or myocardial
infarction should always include assessment of renal function.
Most adverse effects have been mild and transient.
The frequency estimates in the following table were derived from controlled
studies in hypertensive patients in which adverse reactions were either
volunteered by the patient (US studies) or elicited, eg, by checklist (foreign
studies). The reported frequency of elicited adverse effects was higher for both
TENORMIN and placebo-treated patients than when these reactions were
volunteered. Where frequency of adverse effects of TENORMIN and placebo is
similar, causal relationship to TENORMIN is uncertain.
| |
Volunteered
(US Studies) |
|
Total - Volunteered
and Elicited
(Foreign + US Studies) |
| |
Atenolol
(n=164)
% |
Placebo
(n=206)
% |
Atenolol
(n=399)
% |
Placebo
(n=407)
% |
| CARDIOVASCULAR |
| Bradycardia |
3 |
0 |
|
3 |
0 |
| Cold Extremities |
0 |
0.5 |
12 |
5 |
| Postural Hypotension |
2 |
1 |
4 |
5 |
| Leg Pain |
0 |
0.5 |
3 |
1 |
| CENTRAL NERVOUS SYSTEM/NEUROMUSCULAR |
| Dizziness |
4 |
1 |
|
13 |
6 |
| Vertigo |
2 |
0.5 |
2 |
0.2 |
| Light-Headedness |
1 |
0 |
3 |
0.7 |
| Tiredness |
0.6 |
0.5 |
26 |
13 |
| Fatigue |
3 |
1 |
6 |
5 |
| Lethargy |
1 |
0 |
3 |
0.7 |
| Drowsiness |
0.6 |
0 |
2 |
0.5 |
| Depression |
0.6 |
0.5 |
12 |
9 |
| Dreaming |
0 |
0 |
3 |
1 |
| GASTROINTESTINAL |
|
|
|
|
| Diarrhea |
2 |
0 |
3 |
2 |
| Nausea |
4 |
1 |
3 |
1 |
| RESPIRATORY (see Warnings ) |
| Wheeziness |
0 |
0 |
|
3 |
3 |
| Dyspnea |
0.6 |
1 |
6 |
4 |
Acute Myocardial Infarction: In a series of investigations in the
treatment of acute myocardial infarction, bradycardia and hypotension occurred
more commonly, as expected for any beta blocker, in atenolol-treated patients
than in control patients. However, these usually responded to atropine and/or to
withholding further dosage of atenolol. The incidence of heart failure was not
increased by atenolol. Inotropic agents were infrequently used. The reported
frequency of these and other events occurring during these investigations is
given in the following table.
In a study of 477 patients, the following adverse events were reported during
either intravenous and/or oral atenolol administration:
| |
Conventional
Therapy Plus
Atenolol
(n=244) |
Conventional
Therapy
Alone
(n=233)
|
| Bradycardia |
43 |
(18%) |
24 |
(10%) |
| Hypotension |
60 |
(25%) |
34 |
(15%) |
| Bronchospasm |
3 |
(1.2%) |
2 |
(0.9%) |
| Heart Failure |
46 |
(19%) |
56 |
(24%) |
| Heart Block |
11 |
(4.5%) |
10 |
(4.3%) |
| BBB + Major Axis Deviation |
16 |
(6.6%) |
28 |
(12%) |
| Supraventricular Tachycardia |
28 |
(11.5%) |
45 |
(19%) |
| Atrial Fibrillation |
12 |
(5%) |
29 |
(11%) |
| Atrial Flutter |
4 |
(1.6%) |
7 |
(3%) |
| Ventricular Tachycardia |
39 |
(16%) |
52 |
(22%) |
| Cardiac Reinfarction |
0 |
(0%) |
6 |
(2.6%) |
| Total Cardiac Arrests |
4 |
(1.6%) |
16 |
(6.9%) |
| Nonfatal Cardiac Arrests |
4 |
(1.6%) |
12 |
(5.1%) |
| Deaths |
7 |
(2.9%) |
16 |
(6.9%) |
| Cardiogenic Shock |
1 |
(0.4%) |
4 |
(1.7%) |
| Development of Ventricular Septal Defect |
0 |
(0%) |
2 |
(0.9%) |
| Development of Mitral Regurgitation |
0 |
(0%) |
2 |
(0.9%) |
| Renal Failure |
1 |
(0.4%) |
0 |
(0%) |
| Pulmonary Emboli |
3 |
(1.2%) |
0 |
(0%) |
In the subsequent International Study of Infarct Survival (ISIS-1) including
over 16,000 patients of whom 8,037 were randomized to receive TENORMIN
treatment, the dosage of intravenous and subsequent oral TENORMIN was either
discontinued or reduced for the following reasons:
Reasons for Reduced Dosage
| |
IV Atenolol
Reduced Dose
(<5mg) * |
Oral Partial
Dose |
| Hypotension/Bradycardia |
105 |
(1.3%) |
1168 |
(14.5%) |
| Cardiogenic Shock |
4 |
(.04%) |
35 |
(.44%) |
| Reinfarction |
0 |
(0%) |
5 |
(.06%) |
| Cardiac Arrest |
5 |
(.06%) |
28 |
(.34%) |
| Heart Block (> first degree) |
5 |
(.06%) |
143 |
(1.7%) |
| Cardiac Failure |
1 |
(.01%) |
233 |
(2.9%) |
| Arrhythmias |
3 |
(.04%) |
22 |
(.27%) |
| Bronchospasm |
1 |
(.01%) |
50 |
(.62%) |
| *Full dosage was 10 mg and some patients received less
than 10 mg but more than 5 mg. |
During postmarketing experience with TENORMIN, the following have been
reported in temporal relationship to the use of the drug: elevated liver enzymes
and/or bilirubin, hallucinations, headache, impotence, Peyronie's disease,
postural hypotension which may be associated with syncope, psoriasiform rash or
exacerbation of psoriasis, psychoses, purpura, reversible alopecia,
thrombocytopenia, visual disturbances, sick sinus syndrome, and dry mouth.
TENORMIN, like other beta-blockers, has been associated with the development of
antinuclear antibodies (ANA), lupus syndrome, and Raynaud's phenomenon.
POTENTIAL ADVERSE EFFECTS:
In addition, a variety of adverse effects have been reported with other
beta-adrenergic blocking agents, and may be considered potential adverse effects
of TENORMIN.
Hematologic: Agranulocytosis.
Allergic: Fever, combined with aching and sore throat, laryngospasm,
and respiratory distress.
Central Nervous System: Reversible mental depression progressing to
catatonia; an acute reversible syndrome characterized by disorientation of time
and place; short-term memory loss; emotional lability with slightly clouded
sensorium; and, decreased performance on neuropsychometrics.
Gastrointestinal: Mesenteric arterial thrombosis, ischemic colitis.
Other: Erythematous rash.
Miscellaneous: There have been reports of skin rashes and/or dry eyes
associated with the use of beta-adrenergic blocking drugs. The reported
incidence is small, and in most cases, the symptoms have cleared when treatment
was withdrawn. Discontinuance of the drug should be considered if any such
reaction is not otherwise explicable. Patients should be closely monitored
following cessation of therapy. (See DOSAGE AND ADMINISTRATION .)
The oculomucocutaneous syndrome associated with the beta blocker practolol
has not been reported with TENORMIN. Furthermore, a number of patients who had
previously demonstrated established practolol reactions were transferred to
TENORMIN therapy with subsequent resolution or quiescence of the reaction.
Overdosage with TENORMIN has been reported with patients surviving acute
doses as high as 5 g. One death was reported in a man who may have taken as much
as 10 g acutely.
The predominant symptoms reported following TENORMIN overdose are lethargy,
disorder of respiratory drive, wheezing, sinus pause and bradycardia.
Additionally, common effects associated with overdosage of any beta-adrenergic
blocking agent and which might also be expected in TENORMIN overdose are
congestive heart failure, hypotension, bronchospasm and/or hypoglycemia.
Treatment of overdose should be directed to the removal of any unabsorbed
drug by induced emesis, gastric lavage, or administration of activated charcoal.
TENORMIN can be removed from the general circulation by hemodialysis. Other
treatment modalities should be employed at the physician's discretion and may
include:
BRADYCARDIA: Atropine intravenously. If there is no response to vagal
blockade, give isoproterenol cautiously. In refractory cases, a transvenous
cardiac pacemaker may be indicated.
HEART BLOCK (SECOND OR THIRD DEGREE): Isoproterenol or transvenous
cardiac pacemaker.
CARDIAC FAILURE: Digitalize the patient and administer a diuretic.
Glucagon has been reported to be useful.
HYPOTENSION: Vasopressors such as dopamine or norepinephrine (levarterenol).
Monitor blood pressure continuously.
BRONCHOSPASM: A beta 2 stimulant such as isoproterenol or terbutaline
and/or aminophylline.
HYPOGLYCEMIA: Intravenous glucose.
Based on the severity of symptoms, management may require intensive support
care and facilities for applying cardiac and respiratory support.
Dosage and Administration
Hypertension:
The initial dose of TENORMIN is 50 mg given as one tablet a day either alone or
added to diuretic therapy. The full effect of this dose will usually be seen
within one to two weeks. If an optimal response is not achieved, the dosage
should be increased to TENORMIN 100 mg given as one tablet a day. Increasing the
dosage beyond 100 mg a day is unlikely to produce any further benefit.
TENORMIN may be used alone or concomitantly with other antihypertensive
agents including thiazide type diuretics, hydralazine, prazosin, and
alpha-methyldopa.
Angina Pectoris:
The initial dose of TENORMIN is 50 mg given as one tablet a day. If an optimal
response is not achieved within one week, the dosage should be increased to
TENORMIN 100 mg given as one tablet a day. Some patients may require a dosage of
200 mg once a day for optimal effect.
Twenty-four hour control with once daily dosing is achieved by giving doses
larger than necessary to achieve an immediate maximum effect. The maximum early
effect on exercise tolerance occurs with doses of 50 to 100 mg, but at these
doses the effect at 24 hours is attenuated, averaging about 50% to 75% of that
observed with once a day oral doses of 200 mg.
Acute Myocardial Infarction:
In patients with definite or suspected acute myocardial infarction,
treatment with TENORMIN I.V. Injection should be initiated as soon as possible
after the patient's arrival in the hospital and after eligibility is
established. Such treatment should be initiated in a coronary care or similar
unit immediately after the patient's hemodynamic condition has stabilized.
Treatment should begin with the intravenous administration of 5 mg TENORMIN over
5 minutes followed by another 5 mg intravenous injection 10 minutes later.
TENORMIN I.V. Injection should be administered under carefully controlled
conditions including monitoring of blood pressure, heart rate, and
electrocardiogram. Dilutions of TENORMIN I.V. Injection in Dextrose Injection
USP, Sodium Chloride Injection USP, or Sodium Chloride and Dextrose Injection
may be used. These admixtures are stable for 48 hours if they are not used
immediately.
In patients who tolerate the full intravenous dose (10 mg), TENORMIN Tablets
50 mg should be initiated 10 minutes after the last intravenous dose followed by
another 50 mg oral dose 12 hours later. Thereafter, TENORMIN can be given orally
either 100 mg once daily or 50 mg twice a day for a further 6-9 days or until
discharge from the hospital. If bradycardia or hypotension requiring treatment
or any other untoward effects occur, TENORMIN should be discontinued. (See full
prescribing information prior to initiating therapy with TENORMIN Tablets.)
Data from other beta blocker trials suggest that if there is any question
concerning the use of IV beta blocker or clinical estimate that there is a
contraindication, the IV beta blocker may be eliminated and patients fulfilling
the safety criteria may be given TENORMIN Tablets 50 mg twice daily or 100 mg
once a day for at least seven days (if the IV dosing is excluded).
Although the demonstration of efficacy of TENORMIN is based entirely on data
from the first seven postinfarction days, data from other beta blocker trials
suggest that treatment with beta blockers that are effective in the
postinfarction setting may be continued for one to three years if there are no
contraindications.
TENORMIN is an additional treatment to standard coronary care unit therapy.
Elderly Patients or Patients with Renal Impairment:
TENORMIN is excreted by the kidneys; consequently dosage should be adjusted
in cases of severe impairment of renal function. In general, dose selection for
an elderly patient should be cautious, usually starting at the low end of the
dosing range, reflecting greater frequency of decreased hepatic, renal, or
cardiac function, and of concomitant disease or other drug therapy. Evaluation
of patients with hypertension or myocardial infarction should always include
assessment of renal function. Atenolol excretion would be expected to decrease
with advancing age.
No significant accumulation of TENORMIN occurs until creatinine clearance
falls below 35 mL/min/1.73m 2 . Accumulation of atenolol and prolongation of its
half-life were studied in subjects with creatinine clearance between 5 and 105
mL/min. Peak plasma levels were significantly increased in subjects with
creatinine clearances below 30 mL/min.
The following maximum oral dosages are recommended for elderly, renally-impaired
patients and for patients with renal impairment due to other causes:
Creatinine Clearance
(mL/min/1.73m 2 ) |
Atenolol
Elimination Half-Life
(h) |
Maximum Dosage |
| 15-35 |
16-27 |
50 mg daily |
| <15 |
>27 |
25 mg daily |
Some renally-impaired or elderly patients being treated for hypertension may
require a lower starting dose of TENORMIN: 25 mg given as one tablet a day. If
this 25 mg dose is used, assessment of efficacy must be made carefully. This
should include measurement of blood pressure just prior to the next dose
("trough" blood pressure) to ensure that the treatment effect is present for a
full 24 hours.
Although a similar dosage reduction may be considered for elderly and/or
renally-impaired patients being treated for indications other than hypertension,
data are not available for these patient populations.
Patients on hemodialysis should be given 25 mg or 50 mg after each dialysis;
this should be done under hospital supervision as marked falls in blood pressure
can occur.
Cessation of Therapy in Patients with Angina Pectoris:
If withdrawal of TENORMIN therapy is planned, it should be achieved gradually
and patients should be carefully observed and advised to limit physical activity
to a minimum.
How Supplied
TENORMIN Tablets:
Tablets of 25 mg atenolol, NDC 0310-0107,
(round, flat, uncoated white tablets identified with "T" debossed on one side
and 107 debossed on the other side) are supplied in bottles of 100 tablets.
Tablets of 50 mg atenolol, NDC 0310-0105,
(round, flat, uncoated white tablets identified with "TENORMIN" debossed on one
side and 105 debossed on the other side, bisected) are supplied in bottles of
100 tablets.
Tablets of 100 mg atenolol, NDC 0310-0101,
(round, flat, uncoated white tablets identified with "TENORMIN" debossed on one
side and 101 debossed on the other side) are supplied in bottles of 100 tablets.
Storage
Store at controlled room temperature, 20-25°C (68-77°F) [see USP].
Dispense in well-closed, light-resistant containers.
All trademarks are the property of the AstraZeneca group
© AstraZeneca 2002, 2003
Manufactured for:
AstraZeneca Pharmaceuticals LP
Wilmington, DE 19850
By: IPR Pharmaceuticals, Inc.
Carolina, PR 00984
Tenormin patient
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Reviewed: 02/2005
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